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Fc-Dependent Polyclonal Antibodies and Antibodies to Outer Membrane Proteins A and B but Not to Lipopolysaccharide Protect SCID Mice against Fatal Rickettsia conorii Infection

机译：Fc依赖的多克隆抗体和外膜蛋白A和B的抗体而不是脂多糖的抗体可保护SCID小鼠免于致命的立克次体感染

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An emphasis on cellular immunity against Rickettsia has led to neglect of analysis of the role of antibody. The availability of an excellent mouse model of spotted fever rickettsiosis enabled investigation of a potential role of antibody in immunity to Rickettsia conorii. C3H severe combined immunodeficiency (SCID) mice were passively transfused with monoclonal antibodies against rickettsial outer membrane protein A (OmpA), OmpB, or lipopolysaccharide (LPS), polyclonal anti-R. conorii serum, Fab fragments of polyclonal antiserum, or no antibodies and then challenged 48 h later with 10 50% lethal doses (LD50) of R. conorii. All mice that received monoclonal antibodies against OmpA and two of four mice that received monoclonal antibodies against OmpB or polyclonal antisera were completely protected, but the recipients of anti-LPS antibodies or the Fab fragments were not protected. Polyclonal antibody treatment of C3H SCID mice that had been infected with 10 LD50 of R. conorii 4 or 5 days earlier prolonged the life of the infected mice from 10.4 to 22.5 days and resulted in decreased levels of infectious rickettsiae in the spleen and liver 24 and 48 h later. Treatment with protective antibodies resulted in the development of large aggregates of R. conorii antigens in splenic macrophages and intraphagolysosomal rickettsial death and digestion. The kinetics of development of antibodies to R. conorii determined by immunoblotting revealed antibodies to LPS on day 6 and antibodies to OmpA and OmpB on day 12, when recovery from the infection had already occurred. Antibodies to particular epitopes of OmpA and OmpB may protect against reinfection, but they may not play a key role in immunity against primary infection. Antibodies might be useful for treating infections with antibiotic-resistant organisms, and some B-cell epitopes should be included in a subunit vaccine.

机译：对针对立克次体的细胞免疫的强调导致对抗体作用分析的忽视。点状发热立克次体病的优秀小鼠模型的可用性使得能够研究抗体在对立克次氏体免疫中的潜在作用。 C3H重症联合免疫缺陷症（SCID）小鼠被动注射抗立克次氏菌外膜蛋白A（OmpA），OmpB或脂多糖（LPS），多克隆抗R的单克隆抗体。 conorii血清，多克隆抗血清的Fab片段或无抗体，然后在48小时后用10 50％致死剂量（LD50）的conorii沙门氏菌攻击。所有接受抗OmpA单克隆抗体的小鼠和接受抗OmpB单克隆抗体或多克隆抗血清的四只小鼠中的两只均受到完全保护，但抗LPS抗体或Fab片段的接受者未受到保护。在4或5天前用10 LD50的Conorii LD50感染的C3H SCID小鼠多克隆抗体治疗将被感染小鼠的寿命从10.4天延长到22.5天，并导致脾脏和肝脏中感染性立克次体的水平降低24和48小时后。用保护性抗体处理导致脾巨噬细胞中Conorii R. conorii抗原大量聚集，并吞噬溶酶体内立克次体死亡和消化。通过免疫印迹确定的针对Conorii的抗体的发展动力学表明，当感染已经恢复时，第6天的LPS抗体以及第12天的OmpA和OmpB抗体。针对OmpA和OmpB特定表位的抗体可以防止再次感染，但它们可能在抵抗原发性感染的免疫中不发挥关键作用。抗体可能对治疗抗药性微生物感染有用，亚单位疫苗中应包括某些B细胞表位。

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期刊名称 Infection and Immunity
作者
Hui-Min Feng; Ted Whitworth; Juan P. Olano; Vsevolod L. Popov; David H. Walker;
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年(卷),期 2004(72),4
年度 2004
页码 2222–2228
总页数 7
原文格式 PDF
正文语种
中图分类免疫学;病毒传染病;
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专利

1. Fc-Dependent Polyclonal Antibodies and Antibodies to Outer Membrane Proteins A and B, but Not to Lipopolysaccharide, Protect SCID Mice against Fatal Rickettsia conorii Infection [J] . Hui-Min Feng, Ted Whitworth, Juan P. Olano, Infection and immunity . 2004,第4期

机译：Fc依赖性多克隆抗体和外膜蛋白A和B的抗体，而不是脂多糖的抗体，可保护SCID小鼠免遭致命的立克次体感染
2. Outer Membrane Protein-Specific Monoclonal Antibodies Protect SCID Mice from Fatal Infection by the Obligate Intracellular Bacterial PathogenEhrlichia chaffeensis [J] . Julia Shu-yi Li, Eric Yager, Melissa Reilly, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2001,第3期

机译：外膜蛋白特异的单克隆抗体可保护SCID小鼠免于致命的感染，这种感染是由专性细胞内细菌病原菌查菲埃里希氏菌引起的。
3. Outer Membrane Protein-Specific Monoclonal Antibodies Protect SCID Mice from Fatal Infection by the Obligate Intracellular Bacterial Pathogen Ehrlichia chaffeensis [J] . Julia Shu-yi Li, Eric Yager, Melissa Reilly, The journal of immunology . 2001,第3期

机译：外膜蛋白特异性单克隆抗体可保护SCID小鼠免受专性细胞内细菌病原体恰菲埃里希氏菌的致命感染
4. Purification of Dunaliella salina glucose-6-phosphate isomerase (GPI)recombinant proteins in engineering bacteria and preparation of its polyclonal antibody [C] . Lei Zhang, Liuqing Cui, Jie Li, International symposium on pharmacogenomics and the regulation of drug metabolism enzymes and genes. . 2010

机译：工程细菌中杜氏盐藻葡萄糖-6-磷酸异构酶（GPI）重组蛋白的纯化及其多克隆抗体的制备
5. Immunolocalization in SCID mice bearing human tumor using iodine-124 radiolabeled monoclonal antibody JAA-F11. [D] . Yadav, Arti. 2008

机译：使用碘124放射性标记的单克隆抗体JAA-F11在带有人肿瘤的SCID小鼠中进行免疫定位。
6. Combinations of Polyclonal or Monoclonal Antibodies to Proteins of the Outer Membranes of the Two Infectious Forms of Vaccinia Virus Protect Mice against a Lethal Respiratory Challenge [O] . Shlomo Lustig, Christiana Fogg, J. Charles Whitbeck, 1997

机译：痘苗病毒两种感染形式外膜蛋白的多克隆或单克隆抗体的结合可保护小鼠免受致命的呼吸挑战。
7. Fc-Dependent Polyclonal Antibodies and Antibodies to Outer Membrane Proteins A and B, but Not to Lipopolysaccharide, Protect SCID Mice against Fatal Rickettsia conorii Infection [O] . Feng, Hui-Min, Whitworth, Ted, Olano, Juan P., 2004

机译：Fc依赖的多克隆抗体和外膜蛋白A和B的抗体，而不是脂多糖的抗体，可保护SCID小鼠免于致命的立克次体感染
8. Noncovalent Complex Vaccine, Prepared with Detoxified Escherichia coli J5 (RcChemotype) Lipopolysaccharide and Neisseria meningitidis Group B Outer Membrane Protein, Produces Protective Antibodies against Gram-Negative Bacteremia [R] . Bhattacharjee, A. K., Opal, S. M., Taylor, R., 1996

机译：非共价复合疫苗，用解毒的大肠杆菌J5（RcChemotype）脂多糖和脑膜炎奈瑟菌B组外膜蛋白制备，产生针对革兰氏阴性菌血症的保护性抗体

Fc-Dependent Polyclonal Antibodies and Antibodies to Outer Membrane Proteins A and B but Not to Lipopolysaccharide Protect SCID Mice against Fatal Rickettsia conorii Infection

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